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芬戈莫德、特立氟胺和克拉屈滨治疗育龄期女性多发性硬化症:德国药物利用情况和暴露妊娠描述。

Fingolimod, teriflunomide and cladribine for the treatment of multiple sclerosis in women of childbearing age: description of drug utilization and exposed pregnancies in Germany.

机构信息

Department of Clinical Epidemiology, Leibniz Institute for Prevention Research and Epidemiology - BIPS, Bremen, Germany.

Department of Clinical Epidemiology, Leibniz Institute for Prevention Research and Epidemiology - BIPS, Bremen, Germany.

出版信息

Mult Scler Relat Disord. 2022 Nov;67:104184. doi: 10.1016/j.msard.2022.104184. Epub 2022 Sep 14.

Abstract

BACKGROUND

Authorizations of fingolimod, teriflunomide and cladribine were accompanied by risk minimization measures concerning their teratogenic potential. Real-world data on their use are scarce. We aimed to assess trends in the use of fingolimod, teriflunomide and cladribine among women of childbearing age, estimate the number of pregnancies occurring under treatment and explore the occurrence of malformations in newborns exposed during early pregnancy in Germany.

METHODS

Using the German Pharmacoepidemiological Research Database (GePaRD, claims data from ∼20% of the German population), we determined annual age-standardized prevalences of fingolimod, teriflunomide and cladribine use from their authorization until 2019 among women aged 13-49 years (cross-sectional analyses). In longitudinal analyses, we estimated the number of exposed pregnancies by assessing whether there was an overlap between the exposure windows assigned to dispensations and the onset of pregnancy or a dispensation in the first eight weeks of pregnancy. For live births, a mother-baby linkage was performed. All available data of children with in-utero exposure and malformation codes in the first year of life were reviewed to verify the occurrence of congenital malformations.

RESULTS

For fingolimod, the age-standardized prevalence of use per 1,000 females increased from 0.14 in 2011 to 0.46 in 2019; for teriflunomide, from 0.06 in 2013 to 0.28 in 2019; for cladribine, from 0.01 in 2017 to 0.07 in 2019. The proportion of users aged ≤40 years was 60% for fingolimod, 45% for teriflunomide and 65% for cladribine. We identified 136 pregnancies exposed to fingolimod, 50 to teriflunomide and one to cladribine. For fingolimod and teriflunomide, respectively, 72% and 62% of exposed pregnancies ended in a live birth. Mother-newborn linkage was successful in 64 (fingolimod) and 20 (teriflunomide) live-born children. Among these, there were six with relevant malformations (mainly heart defects) for fingolimod and two for teriflunomide.

CONCLUSION

Use of fingolimod, teriflunomide and cladribine among women of childbearing age has substantially increased in Germany. A high proportion of users was in age groups in which pregnancies typically occur. Despite risk minimization measures, early pregnancy exposure to these drugs was observed.

摘要

背景

芬戈莫德、特立氟胺和克拉屈滨的批准伴随着针对其致畸潜力的风险最小化措施。关于它们在现实世界中的使用的数据很少。我们的目的是评估在德国生育年龄的妇女中使用芬戈莫德、特立氟胺和克拉屈滨的趋势,估计治疗期间发生的妊娠数量,并探讨在德国早期妊娠期间暴露于这些药物的新生儿畸形的发生情况。

方法

我们使用德国 Pharmacoepidemiological Research Database (GePaRD,来自约 20%的德国人口的索赔数据),从授权开始到 2019 年,在 13-49 岁的女性中确定了芬戈莫德、特立氟胺和克拉屈滨使用的年度年龄标准化患病率(横截面分析)。在纵向分析中,我们通过评估暴露窗口与妊娠开始或妊娠 8 周内的妊娠重叠情况,估计了暴露于药物的妊娠数量。对于活产,进行了母婴关联。对生命第一年中宫内暴露和畸形代码的所有儿童可用数据进行了审查,以验证先天性畸形的发生情况。

结果

对于芬戈莫德,每 1000 名女性中使用的年龄标准化患病率从 2011 年的 0.14 增加到 2019 年的 0.46;对于特立氟胺,从 2013 年的 0.06 增加到 2019 年的 0.28;对于克拉屈滨,从 2017 年的 0.01 增加到 2019 年的 0.07。芬戈莫德的使用者中年龄≤40 岁的比例为 60%,特立氟胺为 45%,克拉屈滨为 65%。我们发现 136 例妊娠暴露于芬戈莫德,50 例妊娠暴露于特立氟胺,1 例妊娠暴露于克拉屈滨。芬戈莫德和特立氟胺分别有 72%和 62%的暴露妊娠以活产结束。64 名(芬戈莫德)和 20 名(特立氟胺)活产儿成功进行了母婴关联。在这些活产儿中,有 6 名患有相关畸形(主要是心脏缺陷),芬戈莫德有 2 名患有相关畸形。

结论

在德国,生育年龄的妇女中使用芬戈莫德、特立氟胺和克拉屈滨的情况大幅增加。很大一部分使用者处于通常发生妊娠的年龄组。尽管采取了风险最小化措施,但仍观察到这些药物在早期妊娠时的暴露。

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